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免疫细胞与食管癌风险的关联:一项针对东亚人群的孟德尔随机化研究

Association of immune cells and the risk of esophageal cancer: A Mendelian randomization study in a East Asian population.

作者信息

Guo Jinzhou, Si Gao, Si Fuchun

机构信息

Henan University of Chinese Medicine, Zhengzhou, Henan, China.

Laboratory of TCM Syndrome and Prescription Signaling, Academy of Zhongjing, Zhengzhou, Henan, China.

出版信息

Medicine (Baltimore). 2024 May 3;103(18):e38064. doi: 10.1097/MD.0000000000038064.

Abstract

Immunotherapy has been used in esophageal cancer (EC), but the causal relationship between EC and immune cells is not clear. Although the cellular phenotype has been reported as a biomarker for immunotherapy, the biomarker studies for immunotherapy in EC still face great challenges. Comprehensive 2-sample Mendelian randomization (MR) analysis was performed to determine the causal association between immune cell signatures and EC in this study. Based on publicly available genetic data, we explored causal associations between 731 immune cell signatures and EC risk. EC had no statistically significant effect on immunophenotypes. Nine immunophenotype types were positively associated with the risk of EC: CD20-%B cell, CD20% lymphocytes, CD25 on IgD- CD27-, CD25 on IgD+ CD24+, CD27 on IgD+ CD24+, CD28+ CD45RA- CD8br AC, CD3 on TD CD8br, IgD-CD38dim%B cells, and Mo MDSC AC. In addition, a total of 15 immunophenotypes were identified as causally associated with EC. IgD+ CD38- %B cell, IgD- CD24- %lymphocyte, CD19 on IgD- CD38dim, CD20 on IgD+ CD24+, CD62L-myeloid DC AC, CD4+ AC, Lymphocyte %leukocyte, CD3 on HLA-DR+ T cell, CD3 on CD45RA- CD4+, HVEM on naive CD4+ AC, HVEM on CD45RA- CD4+, CD4 on TD CD4+, CD4 on CD4 Treg, and CD4 on CD39+ resting Treg, and CD4 on activated & secreting Treg. Our study has demonstrated the close connection between immune cells and EC by genetic means, thus providing guidance for future clinical research.

摘要

免疫疗法已用于食管癌(EC),但EC与免疫细胞之间的因果关系尚不清楚。尽管细胞表型已被报道为免疫疗法的生物标志物,但EC免疫疗法的生物标志物研究仍面临巨大挑战。本研究进行了全面的两样本孟德尔随机化(MR)分析,以确定免疫细胞特征与EC之间的因果关联。基于公开可用的遗传数据,我们探索了731种免疫细胞特征与EC风险之间的因果关联。EC对免疫表型无统计学显著影响。九种免疫表型类型与EC风险呈正相关:CD20-%B细胞、CD20%淋巴细胞、IgD-CD27-上的CD25、IgD+CD24+上的CD25、IgD+CD24+上的CD27、CD28+CD45RA-CD8br AC、TD CD8br上的CD3、IgD-CD38dim%B细胞和Mo MDSC AC。此外,共鉴定出15种免疫表型与EC存在因果关联。IgD+CD38-%B细胞、IgD-CD24-%淋巴细胞、IgD-CD38dim上的CD19、IgD+CD24+上的CD20、CD62L-髓样DC AC、CD4+AC、淋巴细胞%白细胞、HLA-DR+T细胞上的CD3、CD45RA-CD4+上的CD3、幼稚CD4+AC上的HVEM、CD45RA-CD4+上的HVEM、TD CD4+上的CD4、CD4 Treg上的CD4、CD39+静息Treg上的CD4以及活化和分泌Treg上的CD4。我们的研究通过遗传学方法证明了免疫细胞与EC之间的紧密联系,从而为未来的临床研究提供指导。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/56d8/11062746/f885349218ff/medi-103-e38064-g001.jpg

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